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嗜水气单胞菌II型分泌素组装过程中肽聚糖与ExeAB复合物之间的相互作用。

Interactions between peptidoglycan and the ExeAB complex during assembly of the type II secretin of Aeromonas hydrophila.

作者信息

Howard S Peter, Gebhart Carol, Langen Geoffrey R, Li Gang, Strozen Timothy G

机构信息

Department of Microbiology and Immunology, University of Saskatchewan, Saskatoon, Canada S7N 5E5.

出版信息

Mol Microbiol. 2006 Feb;59(3):1062-72. doi: 10.1111/j.1365-2958.2005.05003.x.

DOI:10.1111/j.1365-2958.2005.05003.x
PMID:16420372
Abstract

Aeromonas hydrophila transports extracellular protein toxins via the type II secretion system, an export mechanism comprised of numerous proteins that spans both the inner and outer membranes. Two components of this secretion system, ExeA and ExeB, form a complex in the inner membrane that functions to locate and/or assemble the ExeD secretin in the outer membrane. In the studies reported here, two-codon insertion mutagenesis of exeA revealed that an insertion at amino acid 495 in the C-terminal region of ExeA did not alter ExeAB complex formation yet completely abrogated its involvement in ExeD secretin assembly and thus rendered the bacteria secretion negative. In silico analysis of protein motifs with similar amino acid profiles revealed that this amino acid is located within a putative peptidoglycan (PG) binding motif in the periplasmic domain of ExeA. Substitution mutations of three highly conserved amino acids in the motif were constructed. In cells expressing each of these mutants, the ability to assemble the ExeD secretin or secrete aerolysin was lost, while ExeA retained the ability to form a complex with ExeB. In in vivo cross-linking experiments, wild-type ExeA could be cross-linked to PG, whereas the three substitution mutants of ExeA could not. These data indicate that PG binding and/or remodelling plays a role in the function of the ExeAB complex during assembly of the ExeD secretin.

摘要

嗜水气单胞菌通过II型分泌系统转运细胞外蛋白毒素,该分泌机制由跨越内膜和外膜的多种蛋白质组成。该分泌系统的两个组分ExeA和ExeB在内膜中形成复合物,其功能是在外膜中定位和/或组装ExeD分泌素。在本文报道的研究中,对exeA进行双密码子插入诱变发现,在ExeA C末端区域的第495位氨基酸处插入并不改变ExeAB复合物的形成,但完全消除了其在ExeD分泌素组装中的作用,从而使细菌分泌呈阴性。对具有相似氨基酸谱的蛋白质基序进行计算机分析发现,该氨基酸位于ExeA周质结构域中一个假定的肽聚糖(PG)结合基序内。构建了该基序中三个高度保守氨基酸的替代突变体。在表达这些突变体的细胞中,组装ExeD分泌素或分泌气溶素的能力丧失,而ExeA保留了与ExeB形成复合物的能力。在体内交联实验中,野生型ExeA可以与PG交联,而ExeA的三个替代突变体则不能。这些数据表明,PG结合和/或重塑在ExeD分泌素组装过程中ExeAB复合物的功能中起作用。

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